photobiomodulation therapy (PBMT) can be applied to a tender area on a subject's body to treat fibromyalgia. A light source device can be contacted to a subject's skin proximal to a tender area on the subject's body. A light signal (with wavelengths from the red to infrared part of the spectrum) can be applied in at least one of a pulsed operating mode, a continuous operating mode, and a super-pulsed operating mode through the light source device to the tender area. The light signal is applied for a time sufficient to stimulate a phototherapeutic response in the tender area to treat fibromyalgia.
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1. A photobiomodulation therapy light source device configured to contact a subject's skin proximal to a tender area on the subject's body and deliver a light signal to the subject through the subject's skin to treat fibromyalgia, the photobiomodulation therapy light source device comprising:
a plurality of clusters of light delivery sources arranged in a ring configuration, each of the clusters of light delivery sources comprising:
a super-pulsed infrared laser configured to operate in a super-pulsed operating mode to generate a first portion of the light signal that comprises an impulse of high intensity with a wavelength from 890-910 nm that emits for a billionth of a second;
a plurality of red light emitting diodes (leds) configured to generate a second portion of the light signal with a wavelength from 600-700 nm in a pulsed operating mode or a continuous operating mode; and
a plurality of infrared leds configured to generate a third portion of the light signal with a wavelength from 810-880 nm in a pulsed operating mode or a continuous operating mode,
wherein the super pulsed infrared laser is surrounded by the plurality of red leds and the plurality of infrared leds; and
at least one permanent magnet configured to provide a constant magnetic field from 5 mT-1 T;
a processing unit preprogrammed with a time duration for application of the light signal to a tender point to treat the tender area; and
a power source.
2. The light source device of
3. The light source device of
4. The light source device of
5. The light source device of
6. The light source device of
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This application is a continuation of U.S. application Ser. No. 16/325,825, filed Feb. 15, 2019, entitled “PHOTOBIOMODULATION THERAPY TO REDUCE THE EFFECTS OF FIBROMYALGIA”, which is a national stage entry of PCT Appl. No. PCT/US2018/027523, filed Apr. 13, 2018, entitled “PHOTOBIOMODULATION THERAPY TO REDUCE THE EFFECTS OF FIBROMYALGIA”, which claims the benefit of U.S. Provisional Application No. 62/485,107, filed Apr. 13, 2017, entitled “SYSTEM OF CONCURRENT USE OF LASERS AND LEDS AND METHOD FOR THE REDUCTION OF PAIN ASSOCIATED WITH FIBROMYALGIA”. This provisional application is hereby incorporated by reference in its entirety for all purposes.
The present disclosure relates generally to photobiomodulation therapy (PBMT) and, more specifically, to systems and methods that apply PBMT to a tender area on a subject's body to treat fibromyalgia (FM).
Fibromyalgia (FM) is a non-inflammatory syndrome characterized by chronic musculoskeletal pain. In patients suffering from FM, the brain and spinal cord process pain sensations abnormally by lowering the threshold at which stimuli cause pain or discomfort. As such, stimuli, which normally would not cause pain, would be amplified in a patient suffering from FM and cause debilitating pain. In many cases, FM can be accompanied by fatigue, sleep, memory, cognitive difficulties, and/or mood issues. Many subjects suffering from fibromyalgia also have tension headaches, migraines, temporomandibular joint (TMJ) disorder, irritable bowel syndrome, interstitial cystitis or painful bladder syndrome, anxiety, and/or depression. These symptoms can be reduced to some degree through medications. Additionally, patients frequently use alternative therapies, like stress management and exercise, to reduce the symptoms as an alternative to or in addition to the medications with varying levels of success. Accordingly, there is a need for a non-pharmacological treatment that can further reduce the symptoms of FM.
The present disclosure relates generally to photobiomodulation therapy (PBMT) and, more specifically, to systems and methods that apply PBMT to a tender area on a subject's body to treat fibromyalgia (FM). PBMT provides a non-pharmacological treatment for fibromyalgia that can be used alone or in combination with medications and/or alternative therapies, like stress management or exercise.
In one aspect, the present disclosure can include a method for applying PBMT to a patient diagnosed with FM to treat FM. A light source device can be contacted to a subject's skin proximal to a tender area on the subject's body. A light signal can be applied in at least one of a pulsed operating mode, a continuous operating mode, and a super-pulsed operating mode through the light source device to the tender area. The light signal is applied for a time sufficient to stimulate a phototherapeutic response in the tender area.
In another aspect, the present disclosure can include a light source device to applying PBMT to a patient diagnosed with FM to treat FM. The light source device can be configured to contact a subject's skin proximal to a tender area on the subject's body and includes a cluster of light delivery sources, a permanent magnet, a processing unit, and a power source. The cluster of light delivery sources can include: a first light source configured to generate a first portion of a light signal with a wavelength from 890-910 nm in a super-pulsed operating mode; a second light source configured to generate a second portion of the light signal with a wavelength from 600-700 nm in a pulsed operating mode or a continuous operating mode; and a third light source configured to generate a third portion of the light signal with a wavelength from 810-880 in the pulsed operating mode or the continuous operating mode. The permanent magnet can provide a constant magnetic field from 5 mT to 1 T. The processing unit can be preprogrammed with a time duration for application of the light signal to the tender area.
The foregoing and other features of the present disclosure will become apparent to those skilled in the art to which the present disclosure relates upon reading the following description with reference to the accompanying drawings, in which:
Unless otherwise defined, all technical terms used herein have the same meaning as commonly understood by one of ordinary skill in the art to which the present disclosure pertains.
In the context of the present disclosure, the singular forms “a,” “an” and “the” can also include the plural forms, unless the context clearly indicates otherwise.
As used herein, the terms “comprises” and/or “comprising” can specify the presence of stated features, steps, operations, elements, and/or components, but do not preclude the presence or addition of one or more other features, steps, operations, elements, components, and/or groups.
As used herein, the term “and/or” can include any and all combinations of one or more of the associated listed items.
Additionally, although the terms “first,” “second,” etc. may be used herein to describe various elements, these elements should not be limited by these terms. These terms are only used to distinguish one element from another. Thus, a “first” element discussed below could also be termed a “second” element without departing from the teachings of the present disclosure. The sequence of operations (or acts/steps) is not limited to the order presented in the claims or figures unless specifically indicated otherwise.
As used herein, the term “photobiomodulation” refers to the application of a light signal to a portion of a subject's body to induce a phototherapeutic response in cells within the portion of the subject's body.
As used herein, the term “photobiomodulation therapy (PBMT)” refers to a drug-free, non-invasive treatment procedure, in which a light signal is applied to a certain region of a subject's body to treat a certain medical condition (e.g., pain, injury, disorder, disease, or the like) via a phototherapeutic response. In some instances, PBMT can be used alone to induce a phototherapeutic response, but in other instances, PBMT can be used in combination with medications and/or alternative therapies, like stress management or exercise, to achieve a more favorable treatment outcome.
As used herein, the term “light signal” refers to light having at least one wavelength. However, the light signal may include a combination of lights having wavelengths that create a synergistic effect when combined and improve the percentage of available light at greater tissue depths. In some instances, the wavelengths can be within a wavelength range of 600-1100 nm. For example, the wavelengths can include at least one wavelength corresponding to the visible range of the electromagnetic spectrum (e.g., red light) and at least one wavelength corresponding to the near-infrared or infrared range of the electromagnetic spectrum.
As used herein, the term “light source device” refers to a mechanical implement that can deliver a light signal of PMBT to a portion of the subject's body. Examples of the light source device include a probe, a flexible array device, or the like.
As used herein, the term “light source” refers to a component of a light source device that delivers one or more lights of different wavelengths. For example, the light source can be a low-level laser source (e.g., a laser light emitting diode (LED)) that generates coherent light. The low-level laser source can operate in a super pulsed mode that generates ultrashort pulses with a high peak power and minimal heat. As another example, the light source can be an incoherent light source, such as a traditional LED or light bulb. The incoherent light source can operate in a pulsed mode and/or a continuous mode.
As used herein, the term “phototherapeutic response” refers to a biological response to application of PBMT to a portion of the subject's body. The biological response can be the creation of a neural blockade to block one or more nocioreceptive pathways to improve a subject's sensitivity to pain.
As used herein, the term “tender area” refers to a portion of a subject's body that experiences pain or discomfort when touched. In some instances, the tender area can include one or more “tender points”, which refers to an extremely sensitive spot on the body, not on a joint itself, which elicits pain in response to application of pressure. Tender points can occur on both the left and right side of the subject's body and can be located in a low cervical region of the subject's body, a second rib of the subject's body, an occiput region of the subject's body, a trapezius muscle of the subject's body, a supraspinatus region of the subject's body, a lateral epicondyle region of the subject's body, a gluteal region of the subject's body, a greater trochanter region of the subject's body, and knee region of the subject's body.
As used herein, the term “treatment” refers to medical care given to a subject to heal or cure a medical condition, like fibromyalgia. The terms “treatment” and “therapy” can be used interchangeably herein.
As used herein, the term “proximal” refers to a location that is near a target. For example, a device that is located proximal a tender area can be located over the tender area, but need not be directly over the center of the tender area.
As used herein, the term “sufficient” refers to an amount adequate enough to satisfy a condition. For example, “a time sufficient to stimulate a phototherapeutic response in a tender area” can refer to a light signal being applied to the tender area for a time adequate enough to stimulate the phototherapeutic response.
As used herein, the term “direct” refers to the absence of intervening elements. For example, a device that directly contacts a skin surface has no intervening elements between the device and the skin surface. When the term “contact” is used herein, it means “direct contact” unless otherwise stated.
As used herein, the terms “subject” and “patient” can be used interchangeably and refer to any warm-blooded organism including, but not limited to, a human being, a pig, a rat, a mouse, a dog, a cat, a goat, a sheep, a horse, a monkey, an ape, a rabbit, a cow, etc.
The present disclosure relates generally to photobiomodulation therapy (PBMT) and, more specifically, to systems and methods that apply PBMT to a tender area on a subject's body to treat fibromyalgia (FM). PBMT provides a non-pharmacological therapy to patients suffering from FM. The PBMT can be used alone or in combination with a pharmaceutical treatment and/or an alternative treatment (like stress management or exercise) to manage the symptoms of FM.
FM, more often afflicting women, is characterized by chronic, widespread musculoskeletal pain. The pain can be accompanied by fatigue, sleep, memory, cognitive difficulties, and/or mood issues. PBMT can be applied to a tender area in a transcutaneous and non-invasive manner. Tender areas can occur on both the left and right side of the subject's body and can include tender points, which can be located in a low cervical region of the subject's body, a second rib of the subject's body, an occiput region of the subject's body, a trapezius muscle of the subject's body, a supraspinatus region of the subject's body, a lateral epicondyle region of the subject's body, a gluteal region of the subject's body, a greater trochanter region of the subject's body, and knee region of the subject's body. By applying the PBMT to a portion of the subject's body proximal to the tender area, a biological response can be triggered, leading to the creation of a neural blockade to block nocioreceptive pathways. Such a neural blockade improves a subject's sensitivity to pain, leading to an improvement in a subject's overall quality of life.
PBMT provides a non-pharmacological therapy that can be administered to a patient in a non-invasive manner to stimulate a phototherapeutic response. As used herein, a light signal is applied through the skin of a patient suffering from fibromyalgia (FM), to a tender area, to stimulate a phototherapeutic response. In this case, the phototherapeutic response can include a biological response leading to the creation of a neural blockade to block nocioreceptive pathways to improve a subject's sensitivity to pain, thereby treating FM. The neural blockade, for example, can be due to the modulation of gene and/or protein expression associated with pain perception and sensitivity. For example, the gene and/or protein expression can be associated with the metabolism of neurotransmitters (e.g., catecholamines, serotonin, and the like). A gene associated with the metabolism of catecholamines (such as dopamine and norepinephrine) is catechol-O-methyltransferase (COMT), while a gene associated with the metabolism of serotonin is the serotonin transporter gene (5-HTT). Additionally or alternatively, the neural blockade can be aided by increased endorphin production, which act as ligands to downstream opioid-receptors to provide an inhibitory response. In addition, the neural blockade can be provided by a decrease in prostaglandin, which can provide pain regression. The neural blockade can also be due to an increase in blood flow dependent on an increase in nitric oxide to assist healing. The biological response can cause a reduction in the symptoms of fibromyalgia.
While not wishing to be bound by theory, there is strong evidence to suggest that one of the basic mechanisms of PBMT is the acceleration of electron transfer by electromagnetic radiation in the visible and near infrared region of the spectrum, via the modulation of cytochrome c-oxidase (CCO) activity. Traditionally, PBMT has attempted to modulate CCO activity using a single wavelength in the visible and near infrared region of the spectrum. However, the use of such single wavelengths cannot effectively modulate CCO activity since the single wavelength is limited by its specific absorption spectrum. The light signal used herein has a combination of wavelengths, which are used concurrently, providing an overlapping effect of peak activation, which accelerates CCO activity. Additionally, the time of CCO activation is prolonged across the entire therapeutic window by delivering much smaller doses across many wavelengths, rather than a single wavelength of a greater power. The multiple wavelengths enhance adenosine triphosphate (ATP) production, requiring less energy, and provides continual photodissociation of nitric oxide (NO), not only from CCO, but also from intracellular stores like nitrosylated forms of hemoglobin and myoglobin. NO is a potent vasodilator and PBMT can increase the vasodilation due to NO and increases the availability of oxygen to treated cells, and allows for greater traffic of immune cells into tissue, which counteracts inflammatory and immune responses and treats fibromyalgia.
Accordingly, the light signal of the present disclosure includes a combination of individual light waves. The combination enhances each individual wavelength's ability to penetrate the skin, to allow for a greater portion of the available light energy to reach biological targets beneath the surface. Accordingly, the light signal can be configured so that individual light waves (from chosen light sources, with a selected wavelength, with a given power, and the like) within the light signal work constructively to create a synergistic effect. The light signal can be delivered by a light source device that includes a combination of one or more super pulsed lasers (which deliver a desired peak power from an ultrashort pulse with a minimized level of heat accumulated in the patient's tissue), one or more infrared emitting diodes, and one or more light emitting diodes. In some instances, the light source device can include groups of a super pulsed laser, an infrared emitting diode, and a light emitting diode. In other instances, the light source device can include groups of a super pulsed laser, at least three infrared emitting diodes, and at least three light source devices. The use of a super pulsed source can minimize the photo-thermal effect accumulating within the skin surface and target tissue. Additionally, the light source device can include a permanent magnet to provide a static (or constant) magnetic field.
One aspect of the present disclosure can include a system 10 (
The system 10 can include at least a light source device 11 that delivers the PBMT to the dystrophic muscle or muscle group and a controller 12 to deliver inputs to the light source device 11 related to the delivery of the PBMT via a wired connection and/or a wireless connection. The PBMT can be applied to the tender area by a light signal that is generated by a light source device 11. To facilitate the delivery of the light signal to the tender area, the light source device 11 can be shaped so that at least a portion makes contact with the subject's skin proximal to the tender area.
The light source device 11 can be configured in any shape that facilitates contacting a portion of the skin and/or the delivery of the light signal. An example of the light source device 11, including an electronics housing 2001 and a device housing 2002, is shown in
As one example, the light source device 11 can be embodied as an insert 2011 (shown in
As another example, the light source device 11 can be embodied as a probe device 3011 (
The light source device 11 can include at least one light delivery source to generate the light signal at a certain wavelength, with a certain power, in an operating mode. The operating mode can be at least one of a pulsed operating mode, a continuous operating mode, and a super-pulsed operating mode. The light source device 11 can also include a processing unit 14 programmed (e.g., preprogrammed, programmed in response to an input from the controller 12 (which may be in response to an input), or the like) with a time duration for application of the light signal to the tender area (e.g., the time duration can be sufficient to stimulate the phototherapeutic response in the tender area). The processing unit 14 can also be programmed with the certain wavelength, the certain power, and/or the operating mode. In some instances, the light source device 11 can also include a permanent magnet to provide a static (or constant) magnetic field, which can be used to secure the light source device 11 to the area of the subject's skin and/or to affect the light signal. The constant magnetic field can be from 5 mT to 1 T. Additionally, the light source device 11 can also include a power source. The power source, in some instances, can be an internal battery. In other instances, the power source can receive and/or store power from an external source. In some instances, the external source can be associated with the controller 12.
In some instances, the light signal can include a light wave at a single wavelength of light delivered in a certain operating mode. However, in other instances, the light signal can include a combination of a plurality of individual light waves with different wavelengths of light delivered in two or more different operating modes. The combination of individual light waves is advantageous because the individual light waves can work constructively to create a synergistic effect, enhancing each individual wavelength's ability to penetrate the skin, allowing for a greater portion of the available light energy to reach biological targets beneath the surface of the skin.
The plurality of individual light waves can be generated by a plurality of light delivery sources. Accordingly, the light source device 11 can include a plurality of light delivery sources, each configured to deliver light of a certain wavelength, with a given power, in a pulsed operating mode, a continuous operating mode, or a super-pulsed operating mode. One organization of the plurality of light delivery sources is in one or more light delivery source clusters 13 (an example of an individual cluster is shown in
As shown in
Many configurations of each light delivery source cluster 13 are possible. Two examples of possible configurations are set forth, but countless other possibilities exist (including with other light sources), as long as there are one or more L1, one or more L2, one or more L3. One possible configuration of each light delivery source cluster 13 is a 1:1:1 configuration, with L1 (the super-pulsed laser) between L2 (the red source) and L3 (the infrared source). Another possible configuration of each light delivery source cluster 13 is a 1:3:3 configuration with L1 surrounded by three (or more) L2 and three (or more) L3. For example, in this configuration, L2 and L3 can alternate as they are arranged around L1 (e.g., L2 L3 L2 L3 L2 L3 surrounding L1). As another example, L2 and L3 can be grouped together around L1 (e.g., L2 L2 L2 L3 L3 L3). Although not expressly described, other example configurations are possible in the 1:3:3 light delivery source cluster 13. The light delivery source clusters 13 within the same light source device 11 can be configured identically, but need not have identical configurations. For example, a light source device 11 can have three light delivery source clusters, with one a 1:1:1 configuration and the other two 1:3:3 configurations.
Another aspect of the present disclosure can include methods 30, 40 (
The methods 30 and 40 are illustrated as process flow diagrams with flowchart illustrations. For purposes of simplicity, the methods 30 and 40 shown and described as being executed serially; however, it is to be understood and appreciated that the present disclosure is not limited by the illustrated order as some steps could occur in different orders and/or concurrently with other steps shown and described herein. Moreover, not all illustrated aspects may be required to implement the methods 30 and 40. Additionally, one or more elements that implement the methods 30 and 40, such as light source device 11 and/or controller 12 of
Referring now to
At step 34, a light signal can be applied to the tender point. The light signal can be generated in at least one of a pulsed operating mode, a continuous operating mode, and a super-pulsed operating mode. The light signal can include one wave of a single wavelength. However, alternatively, the light signal can include a plurality of individual waves with multiple wavelengths. The combination of the plurality of individual waves can work constructively to create a synergistic effect, enhancing each individual wavelength's ability to penetrate the skin, allowing for a greater portion of the available light energy to reach biological targets beneath the surface of the skin. The light signal is applied for a time sufficient to stimulate a phototherapeutic response in the tender point. At step 36, a phototherapeutic response can be stimulated in the tender points. The phototherapeutic response can trigger a biological response leading to the creation of a neural blockade to block nocioreceptive pathways to improve a subject's sensitivity to pain, leading to an improvement in a subject's overall quality of life
The method 30 continues in
The following example is shown for the purpose of illustration only and is not intended to limit the scope of the appended claims. This experiment demonstrates the promise of photobiomodulation therapy (PBMT) as a non-pharmacological tool for treating fibromyalgia (FM). The PBMT provides a non-pharmacological treatment that does not present harmful side effects, making PBMT a promising tool for treating FM, Additionally, PBMT can be combined with exercise training (EXT) to further reduce pain and improve health-related quality of life as well as functional capacity.
Methods
Study Design and Sample
The study was designed to address two main issues: (Set 1—acute) to investigate an immediate effect of a single session of phototherapy/EXT on chronic pain; (Set 2—chronic) to analyze a long-term (10 weeks) effect of the single session of phototherapy/EXT on chronic pain and other FM symptoms. Set 1 and Set 2 were distinct experiments and performed with independent volunteers.
The volunteers were patients from the three rheumatological centers with a FM diagnosis for an average of 5±9 years and evaluated for medical history, physical examination, and rheumatologic screening. The demographics of the volunteers are shown in Table 1.
TABLE 1
Parameters for PBMT
Set 1
Set 2
Age (years)
35 ± 3
40 ± 2
Height (m)
1.58 ± 1
1.59 ± 1
IMC (kg/m2)
26 ± 5
27 ± 4
Race
Other or Biracial
48
41
White
32
39
Education
Elementary School
14
9
High School
66
71
Employment
Employed
52
50
Unemployed
28
20
Income (R$)
<10,000
9
4
10,000-30,000
67
75
30,000-50,000
4
2
Patients received FM diagnostic scores as reported by the American College of Rheumatology on Fibromyalgia Impact Questionnaire (FIQ). The Research Diagnostic Criteria (RDC) was applied aiming at sleeping-disturbed parameters. The recruitment period was from November 2014 to September 2016. The study was carried out according to the Declaration of Helsinki and was registered at ClinicalTrials.gov and approved by an ethics committee.
All participants reported to have maintained the usual pharmacological therapy. Most of the patients used different doses of paracetamol or amitriptyline, and hypnotics were the least used pharmacological class. There were no dropouts or exclusions following randomization nor any harm or unintended outcomes reported.
The inclusion criteria were women ≥35 years old, 5 years from FM diagnosis, optimized drug management, functionally and cognitive independence, full availability for study protocol, and no contraindication to exercise or/and phototherapy. The exclusion criteria were patients with contraindication to exercise or/and phototherapy, missing more than three treatment sessions, psychiatric disorders, missing teeth or use of dentures, history of face trauma or currently undergoing orthodontic intervention, and presence of any disorder that was confused with FM. Patients were followed through their regular health checkups and drug therapy was continued until the end of the study. The eligible participants were instructed not to change their lifestyles or pharmacological therapies during the study.
A total of 160 patients were eligible for the study, Half of these patients were randomly designated to participate in Set 1, and the other participants were designated to participate in Set 2. The patients in each group were randomly assigned, by an independent researcher, to one of the following groups: control (CON) (only under pharmacological treatment); phototherapy (PHO): patients submitted to phototherapy; exercise training (EXT): patients submitted to exercise training and phototherapy placebo (phototherapy device was turned off as a blinding procedure); phototherapy and exercise training (PHO±EXT).
Blinding Procedure and Interventions
An independent researcher was responsible for programming the phototherapy device, which was turned on (phototherapy)/off (placebo) prior to application. A second researcher guided the exercise training and was blinded for phototherapy and/or placebo procedures. A third researcher was blinded to the allocation of patients and independently assessed the outcomes. The statistical analysis was performed by a fourth researcher, who was blinded to experimental groups. All patients were blinded to whether the laser device was in the on or off mode.
The follow-up intervention was 10 weeks, when patients underwent two treatment sessions for phototherapy, exercise, phototherapy/exercise, and placebo procedure per week, respectively (experimental Set 2). Phototherapy was applied 30 min prior to each exercise session or placebo procedure, and treatment sessions were carried out on Tuesdays and Thursdays. The outcome parameters were evaluated at baseline (prior group randomization) and 48 h after the last day of intervention. Similar intervention route was implemented to Set 1 design; however, only a phototherapy and/or an exercise session was conducted to analyze the impact on pain. These patients were evaluated at baseline and after 24 h.
Phototherapy
The multiple light sources (LLLT and LED) Pain Away/PainCure™ nine-diode cluster device (Multi Radiance Medical®, Solon, Ohio, USA) was applied to 10 tender points, which were reported for pain in all patients (occipital, cervical (near the C7), trapezius, supraspinatus, second costochondral joint, lateral epicondyle, gluteal/sacrum, greater trochanter, and medial knee border). The temporomandibular joint (TMJ, bilaterally) was also irradiated. Each point was irradiated for 300 s, and a 39.3-J total energy was delivered. Phototherapy device properties are shown in Table 2.
TABLE 2
Parameters for PBMT
1 Super-pulsed Infrared Laser Diode
Wavelength (nm)
905
Frequency (Hz)
1000
Peak Power (W)
8.5
Average mean optical
0.9
output (mW)
Power density (mW/cm2)
2.25
Energy density (J/cm2)
0.75
Dose (J)
0.3
Spot size of laser (cm2)
0.4
4 Red LEDs
Wavelength (nm)
640 (±10)
Frequency (Hz)
2
Average optical output (mW) - each
15
Power density (mW/cm2) - each
16.66
Energy density (J/cm2) - each
5
Dose (J) - each
4.5
Spot size of red LED (cm2) - each
0.9
4 Infrared LEDs
Wavelength (nm)
875 (±10)
Frequency (Hz)
16
Average optical output (mW) - each
17.5
Power density (mW/cm2) - each
19.44
Energy density (J/cm2) - each
0.155, 0.447, or 1.497
Dose (J) - each
5.25
Spot size of infrared LED (cm2) - each
0.9
Cluster Probe
Magnetic field (mT)
35
Irradiation time per site (s)
300
Total dose per site (J)
39.3
Aperture of device (cm2)
4
Application mode
Cluster probe held
stationary in skin
contact at 90 degree
angle and with slight
pressure
Exercise Training Protocol
The EXT consisted of stretching and aerobic exercise, twice a week, over 10 weeks. Active static stretching was carried out to induce mild discomfort in the following muscle groups: biceps, trapezius, latissimus dorsi, pectoralis, paraspinal, hamstrings, and quadriceps. Each stretching exercise was performed for three times of 30 s with a 30 s rest between each stretching, which shows to be a common rest interval for stretching exercises. Aerobic training was performed 30 min per session on motor drive movement (model LX-150) without inclination. The load exercise was 75% of age-predicted maximum heart rate (220-age (years)). Aerobic training was carried out on the bases of findings of improving the general symptoms, pain, and quality of life in women with fibromyalgia. Each aerobic exercise session was started immediately after the TMJ exercises.
Outcome Measures
General parameters: General parameters are age, body weight, body mass index, race, educational level, employment, in-come, marital status, and tender point count.
Overall clinical parameters: FIQ was a self-administered instrument to measure anxiety, depression, stiffness, and fatigue. RDC was carried out to determine sleeping disturbance, night awakenings, trouble sleeping, and mouth opening pattern.
Pain-Related Outcome
The pain threshold was analyzed with a digital algometer Instrutherm (DD-200 model). The rubber tip of the device (measuring 1 cm2) was placed in contact with the skin on specific FM tender points and TMA joints. A gradual pressure was applied until the patient reported feeling pain, and the displayed values were then recorded. The processes were executed only once to each point and a 30-s interval was given among the readings. Moreover, visual analog scale (VAS) consisting of a 10-cm rule was applied.
Quality of Life
Parameters were evaluated by a validated Brazilian version of the Medical Outcome study 36-item Short-Form Health Survey (SF-36). The following domains were assessed: physical functioning, role-emotional, role-physical, social functioning, mental health, vitality, and general health. The score ranged from 0 to 100, where a higher score represents a better quality of life.
Analysis
Data were analyzed with SPSS Statistics software, version 13.0. The Shapiro Wilk test was carried out to determine a data distribution. Comparisons among the groups were based on analysis of the magnitude of change from the baseline to the end of the interventions (Δ %). The comparisons were analyzed by the Kruskal-Wallis test and post hoc analysis by the Dunn test. The choice of test was established based on the data distribution.
Results
The following results demonstrate the acute and chronic repercussions of PBMT and EXT on pain sensitivity and quality of life of FM patients. The results indicate that the combination of super-pulsed laser and visible red and infrared LED therapy can significantly improve pain ratings in FM women.
The experimental results for Set 1 are shown in
The experimental results for Set 2 are shown in
VAS was used to determine the pain perception in patients undergoing different interventions in Set 2 (
As shown in
From the above description, those skilled in the art will perceive improvements, changes and modifications. Such improvements, changes and modifications are within the skill of one in the art and are intended to be covered by the appended claims. All patents, patent applications, and publications cited herein are incorporated by reference in their entirety.
Johnson, Douglas, Kanarsky, Max, Leal-Junior, Ernesto
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